Multilayered Reprogramming in Response to Persistent DNA Damage in C. elegans

Diletta Edifizi; Hendrik Nolte; Vipin Babu; Laia Castells-Roca; Michael M Mueller; Susanne Brodesser; Marcus Krüger; Björn Schumacher

doi:10.1016/j.celrep.2017.08.028

Multilayered Reprogramming in Response to Persistent DNA Damage in C. elegans

Cell Rep. 2017 Aug 29;20(9):2026-2043. doi: 10.1016/j.celrep.2017.08.028.

Authors

Diletta Edifizi¹, Hendrik Nolte², Vipin Babu¹, Laia Castells-Roca¹, Michael M Mueller¹, Susanne Brodesser², Marcus Krüger³, Björn Schumacher⁴

Affiliations

¹ Institute for Genome Stability in Aging and Disease, Medical Faculty, University of Cologne, Joseph-Stelzmann-Str. 26, Cologne 50931, Germany; Cologne Excellence Cluster for Cellular Stress Responses in Aging-Associated Diseases and Systems Biology of Aging Cologne, University of Cologne, Joseph-Stelzmann-Str. 26, Cologne 50931, Germany.
² Cologne Excellence Cluster for Cellular Stress Responses in Aging-Associated Diseases and Systems Biology of Aging Cologne, University of Cologne, Joseph-Stelzmann-Str. 26, Cologne 50931, Germany.
³ Cologne Excellence Cluster for Cellular Stress Responses in Aging-Associated Diseases and Systems Biology of Aging Cologne, University of Cologne, Joseph-Stelzmann-Str. 26, Cologne 50931, Germany; Center for Molecular Medicine, University of Cologne, Robert-Koch-Str. 21, 50931 Cologne, Germany.
⁴ Institute for Genome Stability in Aging and Disease, Medical Faculty, University of Cologne, Joseph-Stelzmann-Str. 26, Cologne 50931, Germany; Cologne Excellence Cluster for Cellular Stress Responses in Aging-Associated Diseases and Systems Biology of Aging Cologne, University of Cologne, Joseph-Stelzmann-Str. 26, Cologne 50931, Germany; Center for Molecular Medicine, University of Cologne, Robert-Koch-Str. 21, 50931 Cologne, Germany. Electronic address: bjoern.schumacher@uni-koeln.de.

Abstract

DNA damage causally contributes to aging and age-related diseases. Mutations in nucleotide excision repair (NER) genes cause highly complex congenital syndromes characterized by growth retardation, cancer susceptibility, and accelerated aging in humans. Orthologous mutations in Caenorhabditis elegans lead to growth delay, genome instability, and accelerated functional decline, thus allowing investigation of the consequences of persistent DNA damage during development and aging in a simple metazoan model. Here, we conducted proteome, lipidome, and phosphoproteome analysis of NER-deficient animals in response to UV treatment to gain comprehensive insights into the full range of physiological adaptations to unrepaired DNA damage. We derive metabolic changes indicative of a tissue maintenance program and implicate an autophagy-mediated proteostatic response. We assign central roles for the insulin-, EGF-, and AMPK-like signaling pathways in orchestrating the adaptive response to DNA damage. Our results provide insights into the DNA damage responses in the organismal context.

Keywords: Caenorhabditis elegans; DNA damage response; DNA repair; aging; lipidomics; nucleotide excision repair; proteomics.

MeSH terms

Active Transport, Cell Nucleus / radiation effects
Aging / metabolism
Animals
Caenorhabditis elegans / cytology*
Caenorhabditis elegans / metabolism*
Caenorhabditis elegans / radiation effects
Caenorhabditis elegans Proteins / metabolism
Cell Nucleus / metabolism
Cell Nucleus / radiation effects
Cellular Reprogramming* / radiation effects
DNA Damage*
DNA Repair / radiation effects
Down-Regulation / radiation effects
Ion Transport / radiation effects
Lipid Metabolism / radiation effects
Mutation / genetics
Phosphoproteins / metabolism
Proteolysis / radiation effects
Proteome / metabolism
Proteomics
Starvation / metabolism
Synaptic Transmission / radiation effects
Transcriptome / genetics
Transcriptome / radiation effects
Ultraviolet Rays
Up-Regulation / radiation effects

Substances

Caenorhabditis elegans Proteins
Phosphoproteins
Proteome

Grants and funding

260383/ERC_/European Research Council/International